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'OvMark': a user-friendly system for the identification of prognostic biomarkers in publically available ovarian cancer gene expression datasets

机译:'OvMark':一种用户友好的系统,用于在公开可用的卵巢癌基因表达数据集中识别预后生物标志物

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AbstractBackgroundOvarian cancer has the lowest survival rate of all gynaecologic cancers and is characterised by a lack of early symptoms and frequent late stage diagnosis. There is a paucity of robust molecular markers that are independent of and complementary to clinical parameters such as disease stage and tumour grade.MethodsWe have developed a user-friendly, web-based system to evaluate the association of genes/miRNAs with outcome in ovarian cancer. The OvMark algorithm combines data from multiple microarray platforms (including probesets targeting miRNAs) and correlates them with clinical parameters (e.g. tumour grade, stage) and outcomes (disease free survival (DFS), overall survival). In total, OvMark combines 14 datasets from 7 different array platforms measuring the expression of ~17,000 genes and 341 miRNAs across 2,129 ovarian cancer samples.ResultsTo demonstrate the utility of the system we confirmed the prognostic ability of 14 genes and 2 miRNAs known to play a role in ovarian cancer. Of these genes, CXCL12 was the most significant predictor of DFS (HR = 1.42, p-value = 2.42x10−6). Surprisingly, those genes found to have the greatest correlation with outcome have not been heavily studied in ovarian cancer, or in some cases in any cancer. For instance, the three genes with the greatest association with survival are SNAI3, VWA3A and DNAH12.Conclusions/ImpactOvMark is a powerful tool for examining putative gene/miRNA prognostic biomarkers in ovarian cancer (available at http://glados.ucd.ie/OvMark/index.html). The impact of this tool will be in the preliminary assessment of putative biomarkers in ovarian cancer, particularly for research groups with limited bioinformatics facilities.
机译:摘要背景卵巢癌是所有妇科癌症中存活率最低的疾病,其特征在于缺乏早期症状,且经常晚期诊断。缺乏可靠的分子标记,这些标记与临床参数(例如疾病分期和肿瘤等级)无关并与之互补。方法我们已经开发了一个用户友好的基于Web的系统,用于评估基因/ miRNA与卵巢癌预后的关系。 OvMark算法结合了来自多个微阵列平台(包括靶向miRNA的探针集)的数据,并将其与临床参数(例如肿瘤分级,分期)和预后(无疾病生存期(DFS),总生存期)相关联。总共,OvMark结合了来自7个不同阵列平台的14个数据集,这些数据测量了2,129个卵巢癌样品中约17,000个基因和341个miRNA的表达。结果为了证明该系统的实用性,我们确认了14个基因和2个已知在卵巢癌中起作用的miRNA的预后能力。在这些基因中,CXCL12是DFS的最重要预测因子(HR = 1.42,p值= 2.42x10-6)。令人惊讶的是,尚未在卵巢癌或某些癌症的某些情况下对那些与结果具有最大相关性的基因进行大量研究。例如,与生存关联最大的三个基因是SNAI3,VWA3A和DNAH12。结论/影响OvMark是检查卵巢癌中假定的基因/ miRNA预后生物标志物的强大工具(可从http://glados.ucd.ie/OvMark/index.html获得)。该工具的影响将在卵巢癌中可能的生物标记物的初步评估中,特别是对于生物信息学设施有限的研究小组而言。

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